TREC和KREC T-和b细胞受体重排产物在先天性免疫错误患者中的诊断意义

Q4 Medicine
Евгения Александровна Полякова, М.В. Стёганцева, И. Е. Гурьянова, Д.В. Луцкович, Е.Я. Скоповец, А.В. Любушкин, Т. П. Володащик, В. И. Казак, Ю. В. Скибо, М.В. Белевцев, E. A. Polyakova, M. Stegantseva, I. Guryanova, Dmitry V. Lutskovich, K. Skapavets, A. Liubushkin, T. Volodashchik, Victoria I. Kazak, Yulia V. Skibo, M. V. Belevtsev
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引用次数: 0

摘要

先天性免疫错误,如儿童原发性免疫缺陷,是公共卫生的一个重大问题,不可否认,通过创造新的、有效的方法来早期发现涉及免疫机制的疾病,改善这种病理的实验室诊断是很重要的。采用ROC分析评估多重实时荧光定量PCR检测T细胞和b细胞受体DNA环片段(TREC/KREC)拷贝数在基因确定的原发性免疫缺陷患者中的诊断意义。检测年龄为0.0(0 ~ 15.0)岁的健康儿童(n = 98)和年龄为7.2(0.1 ~ 18.0)岁的遗传确诊原发性免疫缺陷患者(n = 95)的外周血DNA样本。现已证实,测定T细胞和B细胞受体重排产物(TREC和KREC)的数量对严重的联合免疫缺陷、染色体不稳定综合征如共济失调性血管扩张症和尼梅亨综合征、免疫失调相关疾病、无球蛋白血症具有很高的诊断意义。测定TREC和KREC对非淋巴细胞功能障碍的免疫缺陷或不影响T和b细胞受体基因重排的疾病(如Wiskott-Aldrich综合征和慢性肉芽肿病)没有帮助。通过检测TREC, KREC具有较高的诊断意义,可用于诊断T淋巴细胞和b淋巴细胞减少症相关的先天性免疫错误。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Diagnostic significance of determining TREC and KREC T- and B-cell receptor rearrangement products in patients with inborn immune errors
Inborn immunity errors such as primary immunodeficiencies in children represent a significant problem for public health, and it is undeniably important to improve the laboratory diagnosis of this pathology by creating new, effective methods for early detection of disorders involving immune mechanisms.The ROC analysis was used to evaluate the diagnostic significance of determining the copy number of T- and B-cell receptor DNA circle fragments (TREC/KREC) by multiplex real-time PCR in patients with a genetically determined diagnosis of primary immunodeficiency.Peripheral blood DNA samples of healthy children (n = 98) aged 0.0 (0-15.0) years, who constituted the control group, and of patients with genetically confirmed primary immunodeficiency (n = 95) aged 7.2 (0.1-18.0) years were examined.It has been established that determining the number of T and B cell receptor rearrangement products (TREC and KREC) has a high diagnostic significance in severe combined immunodeficiency, chromosomal instability syndromes such as ataxiateleangioectasia and Niimegen syndrome, diseases associated with immune dysregulation, agammoglobulinemia. Determining TREC and KREC is not informative in immunodeficiencies with non-lymphoid cell dysfunction or disorders that do not affect T- and B-cell receptor gene rearrangement such as the Wiskott-Aldrich syndrome and the chronic granulomatous disease.Determining TREC, KREC has a high diagnostic significance and can be applied in diagnosis of congenital immunity errors associated with T- and B-cell lymphopenia.
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